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评价来源于 LigB 细胞外基质结合结构域的新型融合蛋白作为仓鼠模型中钩端螺旋体病疫苗候选物的作用。

Evaluation of novel fusion proteins derived from extracellular matrix binding domains of LigB as vaccine candidates against leptospirosis in a hamster model.

机构信息

Department of Population medicine and Diagnostic Sciences, College of Veterinary Medicine, Cornell University, Ithaca, NY 14853, United States.

出版信息

Vaccine. 2011 Oct 6;29(43):7379-86. doi: 10.1016/j.vaccine.2011.07.070. Epub 2011 Jul 29.

DOI:10.1016/j.vaccine.2011.07.070
PMID:21803087
Abstract

Leptospira binds to host extracellular matrix (ECM) through surface exposed outer membrane proteins called adhesin in order to initiate infection. Of various adhesins present on the surface of the spirochete, Leptospira-immunoglobulin like proteins (Lig proteins) and LipL32 are most abundant, widely distributed among pathogenic serovars and well characterized. Various fragments of Lig proteins (Ligcon4, Ligcon4-7.5, LigBcen2) and C-terminus fragment of LipL32 all of that bind to host ECM were fused, expressed and purified in soluble form as fusion proteins. Four week hamsters were immunized subcutaneously with various fusion proteins emulsified in EMULSIGEN-D adjuvant and subsequently boosted at 3 weeks. The protective efficacy of these novel fusion proteins was evaluated against subsequent challenge with highly virulent L. interrogans serovar Pomona (MLD50-100). Our results indicate that fusion protein based vaccine induced significant protection against acute infection with respect to PBS-adjuvant vaccinated controls as revealed by enhanced survival and reduced pulmonary hemorrhage. Moreover, the protection mediated by these novel proteins was higher than that of conserved region of Lig protein (Ligcon, established protective antigen) and correlated to the level of antibodies. LipL32 failed to impart significant protection, however fusing its immunogenic C-terminus domain to Lig fragments slightly delayed the morbidity of the infected animals. Our results demonstrate that this novel strategy could be promising in developing effective subunit vaccine to combat this zoonotic infection.

摘要

钩端螺旋体通过表面暴露的称为黏附素的外膜蛋白与宿主细胞外基质(ECM)结合,从而引发感染。在螺旋体表面存在的各种黏附素中,钩端螺旋体免疫球蛋白样蛋白(Lig 蛋白)和 LipL32 最为丰富,广泛分布于致病性血清型,并且特征良好。各种 Lig 蛋白片段(Ligcon4、Ligcon4-7.5、LigBcen2)和 LipL32 的 C 末端片段都与宿主 ECM 结合,作为融合蛋白以可溶性形式融合、表达和纯化。将各种融合蛋白与 EMULSIGEN-D 佐剂乳化后,通过皮下免疫 4 周龄仓鼠,随后在 3 周时进行加强免疫。用这些新型融合蛋白进行免疫后的保护效力通过随后用高毒力的波蒙那血清型钩端螺旋体(MLD50-100)进行攻毒来评估。我们的结果表明,与 PBS-佐剂免疫的对照组相比,融合蛋白疫苗在急性感染方面诱导了显著的保护作用,表现为存活率提高和肺出血减少。此外,这些新型蛋白介导的保护作用高于 Lig 蛋白保守区(Ligcon,已确定的保护性抗原),并且与抗体水平相关。然而,LipL32 未能提供显著的保护作用,但其免疫原性 C 末端结构域与 Lig 片段融合后,略微延迟了感染动物的发病时间。我们的结果表明,这种新策略在开发针对这种人畜共患病感染的有效亚单位疫苗方面具有广阔的前景。

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